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首页> 外文期刊>Human Molecular Genetics >Biallelic germline mutations in MYH predispose to multiple colorectal adenoma and somatic G:C-->T:A mutations.
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Biallelic germline mutations in MYH predispose to multiple colorectal adenoma and somatic G:C-->T:A mutations.

机译:MYH中的双等位基因种系突变易患多种大肠腺瘤和体细胞G:C-> T:A突变。

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    摘要

    We have recently demonstrated that inherited defects of the base excision repair gene MYH predispose to multiple colorectal adenomas and carcinoma. Three affected siblings from a single British family were identified as Y165C/G382D compound heterozygotes and both missense mutations were shown to be functionally compromised. Here, we report the identification of seven further unrelated patients with >100 colorectal adenomas (six with colorectal cancer) and biallelic germline mutations in MYH: four were homozygous for truncating mutations, two were homozygous for Y165C and one was a Y165C/G382D compound heterozygote. As predicted from studies of the bacterial and yeast orthologues of MYH, colorectal tumours from affected individuals displayed a significant excess of somatic G:C-->T:A mutations in APC, as compared to sporadic ( chi(2)=242.96, P<10(-20)) or FAP-associated ( chi(2)=194.85, P<10(-20)) colorectal tumours. The sequence immediately downstream of the somatic G:C-->T:A mutations was predominantly AA, irrespective of the nature of the germline MYH mutations. These findings confirm the role of MYH in colorectal adenoma and carcinoma predisposition.
    机译:最近,我们证明了碱基切除修复基因MYH的遗传缺陷易患多种大肠腺瘤和癌。来自一个英国家庭的三个受影响的兄弟姐妹被鉴定为Y165C / G382D复合杂合子,并且两个错义突变均显示出功能受损。在此,我们报告了另外7例不相关的患者的鉴定,这些患者的结直肠癌> 100个(大肠癌6例),MYH中存在双等位基因种系突变:4个为截短突变纯合子,2个为Y165C纯合子,1个为Y165C / G382D复合杂合子。根据对MYH细菌和酵母直向同源物的研究预测,与散发性疾病相比,受影响个体的大肠肿瘤在APC中显示出体细胞G:C-> T:A突变显着过量(chi(2)= 242.96,P <10(-20))或与FAP相关的(chi(2)= 194.85,P <10(-20))大肠肿瘤。与种系MYH突变的性质无关,体细胞G:C-> T:A突变紧邻下游的序列主要是AA。这些发现证实了MYH在结直肠腺瘤和癌易感性中的作用。

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